儿童侵袭性曲霉病和毛霉病的合并:一例报告和多中心研究的结果

Y. Dinikina, E. Shagdileeva, S. Khostelidi, O. Shadrivova, Y. Avdeenko, A. G. Volkova, M. Popova, L. S. Zubarovskaya, T. Bogomolova, S. Ignatyeva, A. Kolbin, M. Belogurova, E. Boychenko, N. Klimko
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引用次数: 1

摘要

目标。探讨儿童侵袭性曲霉病(IA)和毛霉病合并(IAM)的危险因素、病因、临床体征和治疗结果。材料与方法。对圣彼得堡注册的IA患者(1998-2021)进行了回顾性审查,并纳入了IAM患儿。采用EORTC/MSGERG 2019标准对侵袭性真菌病进行诊断和治疗效果评价。我们报告了一例急性淋巴细胞白血病复发儿童急性淋巴细胞性白血病的临床病例。他们占所有侵袭性曲霉病患儿的8% (n = 152)。IAM在4 - 16岁(中位年龄- 11.5岁)患有血液恶性肿瘤和实体瘤的儿童中被诊断出来,主要是女孩(83%)。IAM的主要危险因素是化疗、全身皮质类固醇和/或免疫抑制治疗以及造血干细胞移植引起的淋巴细胞减少(75%,中位22天)和中性粒细胞减少(67%,中位30天)。IA的主要病原为黑曲霉(33%)、空心芽孢霉(33%)和烟曲霉(17%),毛霉-衣原体(50%)和根霉(50%)。根据EORTC/MSGERG 2019标准,83%的患者被诊断为“确诊”毛霉病,17%的患者被诊断为“可能”。在100%的患者中发现“可能”IA。IAM最常见的临床部位是肺(75%)和鼻窦(43%),33%的患者出现多灶累及。83%的IA患者在抗真菌治疗期间发生毛霉病。毛霉菌病的抗真菌治疗率为75%(两性霉素B脂质复合物89%,泊沙康唑78%,卡泊芬净33%),联合抗真菌治疗33%,手术治疗50%;42%的患者采用手术联合抗真菌治疗。总12周生存率为77.8%。手术联合抗真菌治疗可显著提高IAM患儿的生存率(p = 0.023)。8%的IA患儿被诊断为毛霉病。IAM主要发生在化疗、全身皮质类固醇和/或免疫抑制治疗以及造血干细胞移植背景下的血液系统恶性肿瘤(83%)、长期淋巴细胞减少(75%)和中性粒细胞减少(67%)患者中。83%的患者在IA抗真菌治疗期间被诊断为毛霉病。IAM的发展增加了总12周死亡率(50%)。抗真菌治疗联合手术治疗可显著改善IAM预后(p = 0.023)。
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Combination of invasive aspergillosis and mucormycosis in children: a case report and the results of a multicenter study
Objective. To study risk factors, etiology, clinical signs and treatment outcomes of invasive aspergillosis (IA) and mucormycosis combination (IAM) in children. Materials and Methods. A retrospective review of Saint-Petersburg register (1998–2021) of patients with IA was done and children with IAM were included. EORTC/MSGERG 2019 criteria were used for diagnosing and treatment results evaluation of invasive mycosis. We presented a clinical case of IAM in a child with acute lymphoblastic leukemia relapse. Results. A total of 12 children with IAM were included. They accounted 8% of all pediatric patients with invasive aspergillosis (n = 152). IAM was diagnosed in children with hematological malignancies and solid tumors from 4 to 16 years (median age – 11.5 years), mostly in girls (83%). Main risk factors of IAM were prolonged lymphopenia (75%, median 22 days) and neutropenia (67%, median 30 days) due to chemotherapy, systemic corticosteroids and/or immunosuppressive therapy, as well as HSCT. The predominant etiological agents of IA were Aspergillus niger (33%), A. nidulans (33%) and A. fumigatus (17%), of mucormycosis – Lichtheimia corymbifera (50%) and Rhizomucor spp. (50%). Based on EORTC/MSGERG 2019 criteria, «proven» mucormycosis was diagnosed in 83% of patients, «probable» – in 17%. «Probable» IA was found in 100% of patients. The most common clinical sites of IAM were the lungs (75%) and paranasal sinuses (43%), multifocal involvement was revealed in 33% of patients. Mucormycosis developed during antifungal therapy of IA in 83% of patients. Antifungal therapy of mucormycosis received 75% of patients (amphotericin B lipid complex – 89%, posaconazole – 78%, caspofungin – 33%), combined antifungal therapy – 33%, surgery – 50%; combination of surgical and antifungal treatment was used in 42% of patients. The overall 12-week survival was 77.8%. The use of combined surgical and antifungal treatment significantly improved the survival of children with IAM (p = 0.023). Conclusions. Mucormycosis was diagnosed in 8% of children with IA. IAM developed mostly in patients with hematological malignancies (83%), prolonged lymphopenia (75%) and neutropenia (67%) against the background of chemotherapy, systemic corticosteroids and/or immunosuppressive therapy, as well as HSCT. In 83% of patients mucormycosis was diagnosed during antifungal therapy for IA. The development of IAM increased overall 12-week mortality (50%). The combination of antifungal therapy with surgical treatment significantly improved prognosis of IAM (p = 0.023).
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